酒精性肌病：病理生理机制与临床意义

Alcoholic Myopathy: Pathophysiologic Mechanisms and Clinical Implications.

作者信息

Simon Liz, Jolley Sarah E, Molina Patricia E

机构信息

Liz Simon, M.V.Sc., Ph.D., is an Assistant Professor in the Department of Physiology, Alcohol and Drug Abuse Center of Excellence; Sarah E. Jolley, M.D., M.Sc., is an Assistant Professor in the Division of Critical Care Medicine; and Patricia E. Molina, M.D., Ph.D., is the Richard Ashman, Ph.D. Professor and Department Head of Physiology, and Director of the Comprehensive Alcohol-HIV/AIDS Research Center and Alcohol and Drug Abuse Center of Excellence, all at the Louisiana State University Health Sciences Center, New Orleans, Louisiana.

出版信息

Alcohol Res. 2017;38(2):207-217.

PMID:28988574

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5513686/

Abstract

Skeletal muscle dysfunction (i.e., myopathy) is common in patients with alcohol use disorder. However, few clinical studies have elucidated the significance, mechanisms, and therapeutic options of alcohol-related myopathy. Preclinical studies indicate that alcohol adversely affects both anabolic and catabolic pathways of muscle-mass maintenance and that an increased proinflammatory and oxidative milieu in the skeletal muscle is the primary contributing factor leading to alcohol-related skeletal muscle dysfunction. Decreased regenerative capacity of muscle progenitor cells is emerging as an additional mechanism that contributes to alcohol-induced loss in muscle mass and impairment in muscle growth. This review details the epidemiology of alcoholic myopathy, potential contributing pathophysiologic mechanisms, and emerging literature on novel therapeutic options.

摘要

骨骼肌功能障碍（即肌病）在酒精使用障碍患者中很常见。然而，很少有临床研究阐明酒精相关性肌病的意义、机制和治疗选择。临床前研究表明，酒精对维持肌肉质量的合成代谢和分解代谢途径均有不利影响，骨骼肌中促炎和氧化环境增加是导致酒精相关性骨骼肌功能障碍的主要因素。肌肉祖细胞再生能力下降是导致酒精引起肌肉质量损失和肌肉生长受损的另一种机制。本文综述详细介绍了酒精性肌病的流行病学、潜在的病理生理机制以及关于新型治疗选择的最新文献。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9f7/5513686/08da61b99500/arcr-38-2-207f1.jpg

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酒精性肌病：病理生理机制与临床意义

Alcoholic Myopathy: Pathophysiologic Mechanisms and Clinical Implications.

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